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一种用于治疗药物靶向递送的新型表皮生长因子受体肽配体的鉴定与表征

Identification and characterization of a novel peptide ligand of epidermal growth factor receptor for targeted delivery of therapeutics.

作者信息

Li Zonghai, Zhao Ruijiao, Wu Xianghua, Sun Ye, Yao Ming, Li Jinjun, Xu Yuhong, Gu Jianren

机构信息

National Laboratory for Oncogenes and Related Genes, Shanghai Cancer Institute, Medical College of Shanghai Jiao Tong University, Shanghai, China.

出版信息

FASEB J. 2005 Dec;19(14):1978-85. doi: 10.1096/fj.05-4058com.

Abstract

Epidermal growth factor receptor (ErbB1, EGFR) is overexpressed in a variety of human cancer cells. It has been considered as a rational target for drug delivery. To identify novel ligands with specific binding capabilities to EGFR, we screened a phage display peptide library and found an enriched phage clone encoding the amino acid sequence YHWYGYTPQNVI (designated as GE11). Competitive binding assay and Scatchard analysis revealed that GE11 peptide bound specifically and efficiently to EGFR with a dissociation constant of approximately 22 nM, but with much lower mitogenic activity than with EGF. We showed that the peptides were internalized preferentially into EGFR highly expressing cells, and they accumulated in EGFR overexpressing tumor xenografts after i.v. delivery in vivo. In gene delivery studies, GE11-conjugated polyethylenimine (PEI) vectors were less mitogenic, but still quite efficient at transfecting genes into EGFR highly expressing cells and tumor xenografts. Taken together, GE11 is a potentially safe and efficient targeting moiety for selective drug delivery systems mediated through EGFR.

摘要

表皮生长因子受体(ErbB1,EGFR)在多种人类癌细胞中过度表达。它已被视为药物递送的合理靶点。为了鉴定与EGFR具有特异性结合能力的新型配体,我们筛选了一个噬菌体展示肽库,发现了一个编码氨基酸序列YHWYGYTPQNVI(命名为GE11)的富集噬菌体克隆。竞争性结合试验和Scatchard分析表明,GE11肽以约22 nM的解离常数特异性且有效地结合到EGFR,但与表皮生长因子(EGF)相比,其促有丝分裂活性要低得多。我们表明,这些肽优先内化到EGFR高表达细胞中,并且在体内静脉注射后,它们在EGFR过表达的肿瘤异种移植中积累。在基因递送研究中,GE11偶联的聚乙烯亚胺(PEI)载体的促有丝分裂活性较低,但在将基因转染到EGFR高表达细胞和肿瘤异种移植中仍然相当有效。综上所述,GE11是通过EGFR介导的选择性药物递送系统的一种潜在安全且有效的靶向部分。

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